Excitation-transcription coupling in sympathetic neurons and the molecular mechanism of its initiation

In excitable cells, membrane depolarization and activation of voltage-gated Ca2+ (CaV) channels trigger numerous cellular responses, including muscle contraction, secretion, and gene expression. Yet, while the mechanisms underlying excitation-contraction and excitation-secretion coupling have been extensively characterized, how neuronal activity is coupled to gene expression has remained more elusive. In this article, we will discuss recent progress toward understanding the relationship between patterns of channel activity driven by membrane depolarization and activation of the nuclear transcription factor CREB. We show that signaling strength is steeply dependent on membrane depolarization and is more sensitive to the open probability of CaV channels than the Ca2+ entry itself. Furthermore, our data indicate that by decoding CaV channel activity, CaMKII (a Ca2+/calmodulin-dependent protein kinase) links membrane excitation to activation of CREB in the nucleus. Together, these results revealed some interesting and unexpected similarities between excitation-transcription coupling and other forms of excitation-response coupling.